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体外评估酶解油基维生素 C 脂肪酸酯的皮肤渗透性能。

In vitro assessment of skin permeation properties of enzymatically derived oil-based fatty acid esters of vitamin C.

机构信息

Faculty of Technology and Metallurgy, University of Belgrade, Belgrade, Serbia.

Innovation Center of Faculty of Technology and Metallurgy, Belgrade, Serbia.

出版信息

Arch Pharm (Weinheim). 2024 Nov;357(11):e2400538. doi: 10.1002/ardp.202400538. Epub 2024 Sep 13.

DOI:10.1002/ardp.202400538
PMID:39268798
Abstract

Current topical formulations containing vitamin C face limitations in therapeutic effectiveness due to the skin's selective properties that impede drug deposition. Consequently, the widespread use of toxic and irritating chemical permeation enhancers is common. Hereby, we investigated enzymatically derived fatty acid ascorbyl esters (FAAEs) obtained using natural oils for their skin permeation properties using the Strat-M® skin model in a Franz cell diffusion study. By evaluating various cosmetic formulations without added enhancers, we found that emulgel is most suitable for enhancing the cutaneous and transdermal delivery of FAAEs. Furthermore, medium-chain coconut oil-derived FAAEs exhibited faster diffusion rates compared to sunflower oil-based FAAEs with long-side acyl residues, including the commonly applied ascorbyl palmitate. Experimental data were successfully fitted using the Peppas and Sahlin model, which accounted for a lag phase and the combined effect of Fickian diffusion and polymer relaxation. In the case of long-chain esters, the lag phase was prolonged, and the calculated effective diffusion coefficients (D) were lower compared to medium-chain FAAEs. Accordingly, the highest D value was observed for ascorbyl caprylate, being even 60 times higher than for ascorbyl palmitate. These results suggest the emerging potential of emulgel with incorporated coconut oil-derived FAAEs for efficiently delivering vitamin C into the skin.

摘要

目前,含有维生素 C 的局部制剂由于皮肤的选择性特性而在治疗效果上存在局限性,这些特性阻碍了药物的沉积。因此,广泛使用有毒和刺激性的化学渗透增强剂是很常见的。在这里,我们研究了使用天然油获得的酶衍生的脂肪酸抗坏血酸酯 (FAAE) 的皮肤渗透特性,使用 Franz 细胞扩散研究中的 Strat-M®皮肤模型。通过评估各种没有添加增强剂的化妆品配方,我们发现乳凝胶最适合增强 FAAE 的皮肤和经皮递送。此外,与具有长侧酰基残基的葵花籽油基 FAAE 相比,来源于中链椰子油的 FAAE 表现出更快的扩散速率,包括常用的抗坏血酸棕榈酸酯。实验数据成功地使用 Peppas 和 Sahlin 模型进行拟合,该模型考虑了滞后相以及 Fickian 扩散和聚合物松弛的综合效应。对于长链酯,滞后相延长,计算得到的有效扩散系数 (D) 低于中链 FAAE。因此,对于抗坏血酸辛酸酯观察到最高的 D 值,甚至比抗坏血酸棕榈酸酯高 60 倍。这些结果表明,含有掺入的椰子油衍生的 FAAE 的乳凝胶具有将维生素 C 有效递送至皮肤的潜力。

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